首页> 外文期刊>Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism >uPA modulates the age-dependent effect of brain injury on cerebral hemodynamics through LRP and ERK MAPK.
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uPA modulates the age-dependent effect of brain injury on cerebral hemodynamics through LRP and ERK MAPK.

机译:uPA通过LRP和ERK MAPK调节脑损伤对脑血流动力学的年龄依赖性效应。

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摘要

We hypothesized that urokinase plasminogen activator (uPA) contributes to age-dependent early hyperemia after fluid percussion brain injury (FPI) by activating extracellular signal-related kinase (ERK) mitogen-activated protein kinase (MAPK), leading to histopathologic changes in the underlying cortex. Both cerebrospinal fluid (CSF) uPA and phosphorylation of CSF ERK MAPK was increased at 1 min after FPI in newborn pigs, but was unchanged in juvenile pigs. uPA and phosphorylated ERK MAPK, detectable in sham piglet brain by immunohistochemistry, was markedly elevated and associated with histopathology 4 h after FPI in the newborn but there was minimal staining and histopathology in the juvenile. EEIIMD, a peptide derived from PA inhibitor-1 that does not affect proteolysis, blunted FPI-induced phosphorylation of ERK MAPK. FPI produced pial artery dilation and increased cerebral blood flow at 1 min after insult in the newborn, but not in the juvenile. Antilipoprotein-related protein (LRP) antibody, EEIIMD, a soluble uPA antagonist, and the ERK MAPK antagonist U 0126 inhibited FPI-associated hyperemia. These data indicate that uPA is upregulated after FPI and produces an age-dependent early hyperemia followed by histopathology through an LRP- and ERK MAPK-dependent pathway.
机译:我们假设尿激酶纤溶酶原激活物(uPA)通过激活细胞外信号相关激酶(ERK)丝裂原激活的蛋白激酶(MAPK)导致液压冲击性脑损伤(FPI)后与年龄有关的早期充血,从而导致潜在的组织病理学改变皮层。 FPI后1分钟,新生猪的脑脊液(CSF)uPA和CSF ERK MAPK磷酸化均增加,但未成年猪没有变化。通过免疫组织化学在假仔猪脑中可检测到的uPA和磷酸化的ERK MAPK显着升高,并在新生儿FPI后4小时与组织病理学相关,但在幼年中染色和组织病理学极少。 EEIIMD,一种不影响蛋白水解的PA抑制剂1衍生肽,使FPI诱导的ERK MAPK磷酸化减弱。 FPI在新生儿受伤后1分钟产生了皮层动脉扩张,并增加了脑血流量,但在未成年人中则没有。抗脂蛋白相关蛋白(LRP)抗体EEIIMD(一种可溶性uPA拮抗剂)和ERK MAPK拮抗剂U 0126可抑制FPI相关的充血。这些数据表明,uPA在FPI后上调,并产生年龄依赖性的早期充血,然后通过LRP和ERK MAPK依赖性途径进行组织病理学检查。

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